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level: Level 1 of Chapter 22 : Cutaneous Drug Eruptions

Questions and Answers List

level questions: Level 1 of Chapter 22 : Cutaneous Drug Eruptions

Question	Answer
How is immunological pathogenesis of cutaneous drug reactionss?	• Type I: IgE dependent: urticaria, angioedema, anaphylaxis. Ex: insulin • Type II: cytotoxic reactions: hemolysis, purpura. Ex: peni, cerebral, sulfa drugs, rifampicin • Type III: IC: Vasculitis, serum sickness, urticaria Ex: quinine, chlorpromazine, salicylates, sulfonamides • Type IV: Delayed HS: eczema, rash, photoallergy. Ex: topical (neomycin, ketoprofen)
How are cutaneous drug reactions?	• It is always careful to consider drugs as a cause of a rash • Most cutaneous drug reactions are inflammatory, generalized and symmetric • Diagnosis is established by their clinical features, including morphology and timing • Histology (skin biopsy) can be helpful • Document the drug reaction in the patient's chart with the medication and description of the reaction
What are most common drug reactions?	• Exanthematous drug reaction • Fixed drug eruption • Urticaria • Photosensitive drug reaction • Drug related eosinophilia with systemic syndrome (DRESS) • Epidermal necrolysis: Stevens-Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN)
What are benign drug reactions?	• Rash • Urticaria • Photosensitivity • Fixed drug eruption
What are immediate vs delayed reactions?	• Classification of drug induced cutaneous reaction according to timing: • Immediate reactions: occur less than 1h of the last administered dose: urticaria, angioedema, anaphylaxis • Delayed reactions: occur more than 1h but usually more than 6h and occasionally weeks to months after the start of administration: Exanthematous eruption, FDE, SJS, TEN, vasculitis
How is non-immunological pathogenesis of cutaneous drug reactions?	• Dose: nasal spray containing silver nitrate. anticoagulants and purpura • Secondary side effects: cyclophosphamide and alopecia • Direct effect on mast cells: aspirin, NSAIDs, Phototoxicity
What are roles of allergy in drug reactions?	• Allergy testing are limited value in evaluating adverse cutaneous reactions to medications • Penicillin is the exception to this rule: pencillin skin testing is the preferred method to evaluate a possible type I - IgE mediated penicillin allergy (urticaria due to peni) • This test also includes the major and minor determinant mixes (metabolites of peni)
How is a complete drug hx done?	The seven I's • Instilled (eye drops, ear drops) • Inhaled (steroids, β adrenergic) • Ingested (capsules, tablets, syrups) • Inserted (suppositories) • Injected (IM, IV) • Incognito (herbs, homeopathic, vitamins, nontraditional medicine, OTC) • Intermittent (medications not mentionned)
What are risk factors of drug reactions?	• Female • Prior history of drug reaction • Recurrent drug exposure: repeated courses of drug therapy with the same drugs are associated with higher rates of adverse drug reactions • HLA-B type: 1502 (carbamazepine and SJS/TEN) 5701 (abacavir and Dress), 5801 (allopurinol and SJS/TEN) • Reactions to aminopenicillin in EBV infection • HIV+ patients have high rate of dermatologic skin reactions to drug as to sulfones and other drugs
How is drug timeline reaction?	• Timing of drug initiation with relation to the rash onset • Preparing a drug timeline could be helpful in this process • Start with the onset of the rash at Day 0 then work backwards and forwards • For the exanthematous drug eruption the initiation of the medication is often 7 to 10 days before first onset and shorter (24-48h) for repeat exposures
What are exanthematous drug eruptions?	• The most common of all cutaneous drug eruptions (90%) • Limited to the skin (no mucous lesions) • Erythematous macules and papules appear on the trunk and spread centrifugally to the extremities with a symmetric fashion • Pruritus and mild fever may be present • Rash appears 7 to 10 days after drug initiation if it is the first episode, 24 to 48h after repeat drug initiation
How is clinical course and tx of exanthematous drug reactions?	• Resolves in a few days to a week after the medication is stopped • May continue the medication safely if the eruption is not too severe and the medication cannot be substituted • Resolves without sequelae (scaling, desquamation) • Treatment: topical steroids, oral antihistamines and reassurance
What are fixed drug eruptions?	• FDE is characterized by the formation of one or more round or oval patches or plaques that will recur at the same site (fixed) with reexposure to the drug • Common drug culprits include: tetracyclines, metronidazole, phenolphtaleine, sulfonamide, barbituriques, NSAID's, salicylate, food coloring (yellow)
How is FDE tx?	• Lesions will resolve days to weeks after the drug is discontinued • Postinflammatory hyperpigmentation (PIH) may persist beyond this time frame • Non-eroded FDE can be treated with a potent topical corticosteroid ointment • Eroded cutaneous FDE can be treated with a protective antibacterial ointment and a dressing untill the skin reepithelialisation • Adress pain especially for mucosal lesions
What is urticaria?	• Lesions will resolve days to weeks after the drug is discontinued • Postinflammatory hyperpigmentation (PIH) may persist beyond this time frame • Non-eroded FDE can be treated with a potent topical corticosteroid ointment • Eroded cutaneous FDE can be treated with a protective antibacterial ointment and a dressing untill the skin reepithelialisation • Adress pain especially for mucosal lesions
What is photosensitivity?	• History: occurred a few hours after sun exposure. • Location on the uncovered areas • Photoallergy: eczema patient areas, sometimes extension on the covered areas and minimal exposures (very down DEM) actuation • Phototoxicity: doses of medication and dependent UVA: Actinic Erythema, bubbles, Onycholysis • Endogenous: metabolic (Porphyria), lupus, idiopathic (Burns) • Contact: plants, perfumes, topical medications...
How is natural hx of photosensitivity?	Occurs few hours after sunexposure. Located on sunexposed areas Photoallergy: eczema of suexposed areas with spreading on covered areas, induced by minimal sunexposure (MED very low) Phototoxicity: doses of drugs UVA dependent: actinic erythema, blisters.. Systemic : metabolic (porphyrias), lupus, polymorphous light eruption.
What is drug-induced HS syndrome?	• Syn. Drug related eosinophilia with systemic syndrome (DRESS) • Skin eruption with systemic symptoms and internal organ involvement (heart, kidney, liver) • Typical signs and symptoms: exanthem, erythematous centrofacial swelling, fever, malaise, lymphadenopathy, ad involvement of other organs (liver, kidneys) • >70% have eosinophilia • Liver function tests (LFTs) abnormalities and/or hepatosplenomegaly are helpful diagnostic clues
How is clinical course of DIHS?	• Signs and symptoms start at the 3rd week (1 to 12 weeks) after starting the medication or after increasing the dose • They may persist and recur for many weeks even after cessation of drug treatment • Fatality rate may be up to 10%
How is DIHS tx?	• Stop suspect medication (s) • If not severe: topical steroids and systemic antihistamines, and continue to follow lab values • If severe: systemic steroids (prednisone 1mg/kg/day) and taper very gradually over weeks to months as syndrome can recur as the dose reduces • Severely ill patients may need to be hospilized in an ICU setting
What is steven-johnson's syndrome/ toxic epidermal necolysis?	• SJS and TEN are acute life-threatening mucocutaneous reactions • Characterized by extensive necrosis and detachment of the epidermis and mucosal surfaces • They represent similar processes but differ in severity based on body surface area (BSA) that is involved • SJS/TEN is a dermatologic emergency • Mortality rate varies from 5-12%, and >20% for TEN • Old age, significant comorbid conditions, and greater extent of skin involvement correlate with poor prognosis
What are drugs causing SJS/TEN?	• Over 100 different drugs have been associated with SJS/TEN. The most high risk are: SATAN • Sulfa ATB, sulfasalazine • Allopurinol • Tetracyclines, thiacetazone • Anticonvulsivants (carbamazepine, lamotrigine, phenobarbital, phenytoin) • NSAID's • Nevirapine
How is clinical presentation of SJS?	• Onset wihin 8 weeks after drug initiation • Fever, headache, rhinitis, and myalgias may precede mucocutaneous lesions by 1-3 days • Eruption is initially symmetric and distributed on the face, upper trunk, and proximal extremities • Pain is a prominent symptom due to necrosis • Lesions may extend rapidly to the rest of the body
How is hx of SJS lesions?	• Initial skin lesions are erythematous, irregulary shaped, dusky red to purpuric macules (atypical targets), which progressively coalesce • Dark center of atypical target lesions may blister evolving to flaccid blisters • The necrotic epidermis is easily detached at pressure points or by frictional trauma • Patients are classified into 3 groups depending on the BSA: SJS<10% SJS/TEN 10-30% SJS/TEN>30%
How is mucus membrane involvement in SJS?	• Can precede skin eruption • Begins with erythema followed by painful erosions of the oral, ocular, and genital mucosa • A significant percentage of patients with ocular involvement will suffer permanent ocular sequelae, even blindness
What are SJS complications?	• Corneal damage • Oral cavity • GU damage (adhesions, urethral/introital erosions) • Pulmonary damage (bronchitis, bronchiectasis) • Fluid and electrolyte disturbances • Nutrition requirements • Secondary infection (bacteremia, sepsis)
How is SJS tx?	• Early recognition and withdrawal of the offending and supportive care • In case of doubt, all non-life-sustaining drugs should be stopped • Care should be proceed in a burn unit for patients with significant BSA involvement • Multidisciplinary approach • Specific therapies: IV Ig, Cyclosporine, etanercept according to the stage of the disease and the centers experience